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产前可卡因暴露对皮质中间神经元的影响特异性与多巴胺 D1 受体共定位无关。

Specificity of prenatal cocaine exposure effects on cortical interneurons is independent from dopamine D1 receptor co-localization.

机构信息

Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, TN 37232, United States.

出版信息

J Chem Neuroanat. 2010 Jul;39(4):228-34. doi: 10.1016/j.jchemneu.2010.01.002. Epub 2010 Jan 18.

Abstract

Gestational cocaine exposure in a rabbit model leads to a persistent increase in parvalbumin immunoreactive cells and processes, reduces dopamine D1 receptor coupling to Gsalpha by means of improper trafficking of the receptor, changes pyramidal neuron morphology, and disrupts cognitive function. Here, experiments investigated whether changes in parvalbumin neurons were specific, or extended to other subpopulations of interneurons. Additionally, we examined dopamine D1 receptor expression patterns and its overlap with specific interneuron populations in the rabbit prefrontal cortex as a possible correlate for alterations in interneuron development following prenatal cocaine exposure. Analysis of calbindin and calretinin interneuron subtypes revealed that they did not exhibit any differences in cell number or process development. Thus, specific consequences of prenatal cocaine in the rabbit appear to be limited to parvalbumin-positive interneurons. Dopamine D1 receptor expression did not correlate with the selective effects of cocaine exposure, however, as both parvalbumin and calbindin cell types expressed the receptor. The findings suggest that additional, unique properties of parvalbumin neurons contribute to their developmental sensitivity to in utero cocaine exposure.

摘要

在兔模型中,妊娠期可卡因暴露会导致 GABA 能中间神经元的 parvalbumin 免疫反应性细胞和突起持续增加,通过受体的不当转运减少多巴胺 D1 受体与 Gsalpha 的偶联,改变锥体神经元形态,并破坏认知功能。在这里,实验研究了 parvalbumin 神经元的变化是否具有特异性,或者是否扩展到其他中间神经元亚群。此外,我们还研究了多巴胺 D1 受体在兔前额叶皮层中的表达模式及其与特定中间神经元群体的重叠,作为产前可卡因暴露后中间神经元发育改变的可能相关因素。钙结合蛋白和钙调蛋白中间神经元亚型的分析表明,它们在细胞数量或突起发育方面没有差异。因此,兔产前可卡因的特定后果似乎仅限于 parvalbumin 阳性中间神经元。然而,多巴胺 D1 受体的表达与可卡因暴露的选择性影响无关,因为 parvalbumin 和钙结合蛋白两种细胞类型都表达了该受体。这些发现表明,parvalbumin 神经元的其他独特特性导致了它们对宫内可卡因暴露的发育敏感性。

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